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Characterization of the disassembly and reassembly of the HBV glycoprotein surface antigen a pliable nanoparticle vaccine platform

机译:HBV糖蛋白表面抗原的拆卸和重新组装的特性一种柔软的纳米颗粒疫苗平台

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摘要

While nanoparticle vaccine technology is gaining interest due to the success of vaccines like those for the human papillomavirus that is based on viral capsid nanoparticles, little information is available on the disassembly and reassembly of viral surface glycoprotein-based nanoparticles. One such particle is the hepatitis B virus surface antigen (sAg) that exists as nanoparticles. Here we show, using biochemical analysis coupled with electron microscopy, that sAg nanoparticle disassembly requires both reducing agent to disrupt intermolecular disulfide bonds, and detergent to disrupt hydrophobic interactions that stabilize the nanoparticle. Particles were otherwise resistant to salt and urea, suggesting the driving mechanism of particle formation involves hydrophobic interactions. We reassembled isolated sAg protein into nanoparticles by detergent removal and reassembly resulted in a wider distribution of particle diameters. Knowledge of these driving forces of nanoparticle assembly and stability should facilitate construction of epitope-displaying nanoparticles that can be used as immunogens in vaccines.
机译:尽管由于基于病毒衣壳纳米粒子的人乳头瘤病毒等疫苗的成功,纳米粒子疫苗技术引起了人们的兴趣,但有关基于病毒表面糖蛋白的纳米粒子的拆卸和重新组装的信息却很少。一种这样的颗粒是作为纳米颗粒存在的乙型肝炎病毒表面抗原(sAg)。在这里,我们使用生化分析和电子显微镜显示,sAg纳米颗粒的分解既需要还原剂破坏分子间二硫键,也需要去污剂破坏稳定纳米颗粒的疏水相互作用。否则颗粒对盐和尿素具有抗性,表明颗粒形成的驱动机制涉及疏水相互作用。我们通过去污剂的去除将重组的sAg蛋白重组为纳米颗粒,并进行重组,从而使粒径分布更广。对纳米颗粒组装和稳定性的这些驱动力的了解应有助于构建可在疫苗中用作免疫原的表位展示纳米颗粒。

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